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用于研究反刍动物天然宿主中蓝舌病病毒和绵羊边界病病毒发病机制的可靠且标准化动物模型,特别强调胎盘传播。

Reliable and Standardized Animal Models to Study the Pathogenesis of Bluetongue and Schmallenberg Viruses in Ruminant Natural Host Species with Special Emphasis on Placental Crossing.

机构信息

CARE-FEPEX experimental station, Fundamental and Applied Research for Animals & Health (FARAH) Center, Faculty of Veterinary Medicine, University of Liege, 4000 Liege, Belgium.

Research Unit in Epidemiology and Risk Analysis Applied to Veterinary Sciences (UREAR-ULg), Fundamental and Applied Research for Animals & Health (FARAH) Center, Faculty of Veterinary Medicine, University of Liege, 4000 Liege, Belgium.

出版信息

Viruses. 2019 Aug 15;11(8):753. doi: 10.3390/v11080753.

DOI:10.3390/v11080753
PMID:31443153
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6722754/
Abstract

Starting in 2006, bluetongue virus serotype 8 (BTV8) was responsible for a major epizootic in Western and Northern Europe. The magnitude and spread of the disease were surprisingly high and the control of BTV improved significantly with the marketing of BTV8 inactivated vaccines in 2008. During late summer of 2011, a first cluster of reduced milk yield, fever, and diarrhoea was reported in the Netherlands. Congenital malformations appeared in March 2012 and Schmallenberg virus (SBV) was identified, becoming one of the very few orthobunyaviruses distributed in Europe. At the start of both epizootics, little was known about the pathogenesis and epidemiology of these viruses in the European context and most assumptions were extrapolated based on other related viruses and/or other regions of the World. Standardized and repeatable models potentially mimicking clinical signs observed in the field are required to study the pathogenesis of these infections, and to clarify their ability to cross the placental barrier. This review presents some of the latest experimental designs for infectious disease challenges with BTV or SBV. Infectious doses, routes of infection, inoculum preparation, and origin are discussed. Particular emphasis is given to the placental crossing associated with these two viruses.

摘要

自 2006 年以来,8 型蓝舌病毒(BTV8)导致了西欧和北欧的一次重大流行病。疾病的规模和传播令人惊讶地高,随着 2008 年 BTV8 灭活疫苗的上市,BTV 的控制得到了显著改善。2011 年夏末,荷兰首次报告了产奶量减少、发热和腹泻的病例群。2012 年 3 月出现了先天性畸形,并鉴定出 Schmallenberg 病毒(SBV),成为在欧洲分布的少数正粘病毒之一。在两次流行病的开始时,人们对这些病毒在欧洲背景下的发病机制和流行病学知之甚少,大多数假设都是基于其他相关病毒和/或世界其他地区推断出来的。需要标准化和可重复的模型来模拟田间观察到的临床症状,以研究这些感染的发病机制,并阐明它们穿过胎盘屏障的能力。本文综述了一些最新的 BTV 或 SBV 感染性疾病挑战的实验设计。讨论了感染剂量、感染途径、接种物制备和来源。特别强调了这两种病毒与胎盘穿越相关的问题。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2ff9/6722754/edbb5aa03895/viruses-11-00753-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2ff9/6722754/edbb5aa03895/viruses-11-00753-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2ff9/6722754/edbb5aa03895/viruses-11-00753-g001.jpg

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